Natural products based on Correa's cascade for the treatment of gastric cancer trilogy:Current status and future perspective
10.1016/j.jpha.2024.101075
- Author:
Wenhao LIAO
1
;
Jing WANG
;
Yuchen LI
Author Information
1. Department of Nephrology,the Key Laboratory for the Prevention and Treatment of Chronic Kidney Disease of Chongqing,Chongqing Clinical Research Center of Kidney and Urology Diseases,Xinqiao Hospital,Army Medical University(Third Military Medical University),Chongqing,400037,China
- Publication Type:Journal Article
- Keywords:
Atrophic gastritis;
Correa's cascade;
Dysplasia;
Gastric carcinoma;
Helicobacter pylori;
Gastric precancerous lesions;
Intestinal metaplasia;
Natural products
- From:
Journal of Pharmaceutical Analysis
2025;15(2):325-341
- CountryChina
- Language:English
-
Abstract:
Gastric carcinoma(GC)is a malignancy with multifactorial involvement,multicellular regulation,and multistage evolution.The classic Correa's cascade of intestinal GC specifies a trilogy of malignant transformation of the gastric mucosa,in which normal gastric mucosa gradually progresses from inactive or chronic active gastritis(Phase Ⅰ)to gastric precancerous lesions(Phase Ⅱ)and finally to GC(Phase Ⅲ).Correa's cascade highlights the evolutionary pattern of GC and the importance of early intervention to prevent malignant transformation of the gastric mucosa.Intervening in early gastric mucosal lesions,i.e.,Phases Ⅰ and Ⅱ,will be the key strategy to prevent and treat GC.Natural products(NPs)have been an important source for drug development due to abundant sources,tremendous safety,and multiple pharmacodynamic mechanisms.This review is the first to investigate and summarize the multi-step effects and regulatory mechanisms of NPs on the Correa's cascade in gastric carcinogenesis.In Phase Ⅰ,NPs modulate Helicobacter pylori urease activity,motility,adhesion,virulence factors,and drug resis-tance,thereby inhibiting H.pylori-induced gastric mucosal inflammation and oxidative stress,and facilitating ulcer healing.In Phase Ⅱ,NPs modulate multiple pathways and mediators regulating gastric mucosal cell cycle,apoptosis,autophagy,and angiogenesis to reverse gastric precancerous lesions.In Phase Ⅲ,NPs suppress cell proliferation,migration,invasion,angiogenesis,and cancer stem cells,induce apoptosis and autophagy,and enhance chemotherapeutic drug sensitivity for the treatment of GC.In contrast to existing work,we hope to uncover NPs with sequential therapeutic effects on multiple phases of GC development,providing new ideas for gastric cancer prevention,treatment,and drug development.
